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Topologically associating domains define the impact of de novo promoter variants on autism spectrum disorder risk.


ABSTRACT: Whole-genome sequencing (WGS) studies of autism spectrum disorder (ASD) have demonstrated the roles of rare promoter de novo variants (DNVs). However, most promoter DNVs in ASD are not located immediately upstream of known ASD genes. In this study analyzing WGS data of 5,044 ASD probands, 4,095 unaffected siblings, and their parents, we show that promoter DNVs within topologically associating domains (TADs) containing ASD genes are significantly and specifically associated with ASD. An analysis considering TADs as functional units identified specific TADs enriched for promoter DNVs in ASD and indicated that common variants in these regions also confer ASD heritability. Experimental validation using human induced pluripotent stem cells (iPSCs) showed that likely deleterious promoter DNVs in ASD can influence multiple genes within the same TAD, resulting in overall dysregulation of ASD-associated genes. These results highlight the importance of TADs and gene-regulatory mechanisms in better understanding the genetic architecture of ASD.

SUBMITTER: Nakamura T 

PROVIDER: S-EPMC10879036 | biostudies-literature | 2024 Feb

REPOSITORIES: biostudies-literature

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Topologically associating domains define the impact of de novo promoter variants on autism spectrum disorder risk.

Nakamura Takumi T   Ueda Junko J   Mizuno Shota S   Honda Kurara K   Kazuno An-A AA   Yamamoto Hirona H   Hara Tomonori T   Takata Atsushi A  

Cell genomics 20240126 2


Whole-genome sequencing (WGS) studies of autism spectrum disorder (ASD) have demonstrated the roles of rare promoter de novo variants (DNVs). However, most promoter DNVs in ASD are not located immediately upstream of known ASD genes. In this study analyzing WGS data of 5,044 ASD probands, 4,095 unaffected siblings, and their parents, we show that promoter DNVs within topologically associating domains (TADs) containing ASD genes are significantly and specifically associated with ASD. An analysis  ...[more]

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